4.8 Article

Enterically derived high-density lipoprotein restrains liver injury through the portal vein

SCIENCE (2021)

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Journal

SCIENCE
Volume 373, Issue 6553, Pages 410-+

Publisher

AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/science.abe6729

Keywords

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Categories

Multidisciplinary Sciences

Funding

  1. National Institutes of Health (NIH) [R01DK119147, AI0499653]
  2. National Research Foundation (NRF) of Korea [2021R1C1C1004023]
  3. NIH [T32DK077653, RO1HL127649, HL138908, P30 DK052574]
  4. AHA Career Development Award [AHA:18CDA34110273]
  5. Lawrence C. Pakula, MD IBD Research Fellowship
  6. Children's Discovery Institute of Washington University [CDI-CORE-2015-505, CDI-CORE-2019813]
  7. Foundation for Barnes-Jewish Hospital [3770]
  8. WU Institute of Clinical and Translational Sciences [NCATS UL1 TR000448]
  9. Mass Spectrometry Research Resource [NIGMS P41 GM103422, R24GM136766]
  10. Siteman Comprehensive Cancer Center [NCI P30 CA091842]
  11. NCI Cancer Center [P30 CA91842]
  12. ICTS/CTSA grant from the National Center for Research Resources (NCRR) [UL1TR002345]
  13. National Research Foundation of Korea [2021R1C1C1004023] Funding Source: Korea Institute of Science & Technology Information (KISTI), National Science & Technology Information Service (NTIS)

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Research shows that HDL3 derived from the intestine can enter the bloodstream through the portal vein, preventing the binding of lipopolysaccharide and inflammatory activation of liver macrophages, thereby protecting the liver from injury caused by gut-derived LPS.
The biogenesis of high-density lipoprotein (HDL) requires apoA1 and the cholesterol transporter ABCA1. Although the liver generates most of the HDL in the blood, HDL synthesis also occurs in the small intestine. Here, we show that intestine-derived HDL traverses the portal vein in the HDL3 subspecies form, in complex with lipopolysaccharide (LPS)-binding protein (LBP). HDL3, but not HDL2 or low-density lipoprotein, prevented LPS binding to and inflammatory activation of liver macrophages and instead supported extracellular inactivation of LPS. In mouse models involving surgical, dietary, or alcoholic intestinal insult, loss of intestine-derived HDL worsened liver injury, whereas outcomes were improved by therapeutics that elevated and depended upon raising intestinal HDL. Thus, protection of the liver from injury in response to gut-derived LPS is a major function of intestinally synthesized HDL.

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